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 Printable version |
Identification of basal-like carcinomas in clinical practice: “triple zero/BRCA1-like” carcinomas |
Bulletin du Cancer. Volume 97, Number 3, 357-63, mars 2010, Synthèse
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 Résumé
Article gratuit
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Author(s) : A Vincent-Salomon, G Macgrogan, E Charaffe-Jauffret, J Jacquemier, L Arnould |
Summary : Basal-like carcinomas represent 10 to 15% of invasive breast carcinomas and have been identified from gene expression studies. Morphologically, these tumors are undifferentiated histopronostic grade 3 carcinomas, identified in clinical practice according to their immunophenotype “triple zero” (estrogen, progesterone and ERBB2 negative) associated with the high molecular weight cytokeratins 5/6/14 and/or EGFR expression. At the molecular level, these tumors harbour nearly 100% P53 mutations, a high rate of PTEN mutations with an AKT pathway’s activation and numerous chromosomal alterations such as gains and losses. They share a high degree of similarity at the morphological, phenotypical and molecular level with BRCA1 tumors that justify the proposal of a different name such as “triple zero/BRCA1 like” carcinomas for sporadic basal-like carcinomas. Indeed, the current “basal-like” name could suggest a myoepithelial cellular origin of such lesions. Furthermore, tumors with such a basal-like immunophenotype constitute a heterogeneous group of tumors encompassing good prognosis tumors such as adenoid cystic and juvenile secretory carcinomas. There is an urgent need for more specific therapies for basal-like/triple zero/BRCA1-like tumors. Therapeutic progresses rely on a better understanding of the molecular alterations that occur in these tumors and the BRCA1 tumors. Indeed, recent clinical trials with PARP inhibitors for basal-like/BRCA1 like tumors should improve the prognosis of these patients and are a direct benefit of a better understanding of the molecular biology of these tumors. |
Keywords : basal-like carcinoma, breast cancer, gene expression profiling, phenotype, PARP inhibitors |
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